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乳腺癌转移的基因组结构:聚焦机制、信号通路及治疗策略

The genomic architecture of metastasis in breast cancer: focus on mechanistic aspects, signalling pathways and therapeutic strategies.

作者信息

Chhichholiya Yogita, Suman Prabhat, Singh Sandeep, Munshi Anjana

机构信息

Department of Human Genetics and Molecular Medicine, Central University of Punjab Bathinda, Punjab, India.

出版信息

Med Oncol. 2021 Jul 16;38(8):95. doi: 10.1007/s12032-021-01547-1.

Abstract

Breast cancer is a multifactorial, heterogeneous disease and the second most frequent cancer amongst women worldwide. Metastasis is one of the most leading causes of death in these patients. Early-stage or locally advanced breast cancer is limited to the breast or nearby lymph nodes. When breast cancer spreads to farther tissues/organs from its original site, it is referred to as metastatic or stage IV breast cancer. Normal breast development is regulated by specific genes and signalling pathways controlling cell proliferation, cell death, cell differentiation and cell motility. Dysregulation of genes involved in various signalling pathways not only leads to the formation of primary tumour but also to the metastasis as well. The metastatic cascade is represented by a multi-step process including invasion of the local tumour cell followed by its entry into the vasculature, exit of malignant cells from the circulation and ultimately their colonization at the distant sites. These stages are referred to as formation of primary tumour, angiogenesis, invasion, intravasation and extravasation, respectively. The major sites of metastasis of breast cancer are the lymph nodes, bone, brain and lung. Only about 28% five-year survival rate has been reported for stage IV breast cancer. Metastasis is a serious concern for breast cancer and therefore, various therapeutic strategies such as tyrosine kinase inhibitors have been developed to target specific dysregulated genes and various signalling pathways involved in different steps of metastasis. In addition, other therapies like hyperbaric oxygen therapy, RNA interference and CRISPR/Cas9 are also being explored as novel strategies to cure the stage IV/metastatic breast cancer. Therefore, the current review has been compiled with an aim to evaluate the genetic basis of stage IV breast cancer with a focus on the molecular mechanisms. In addition, the therapeutic strategies targeting these dysregulated genes involved in various signalling pathways have also been discussed. Genome editing technologies that can target specific genes in the affected areas by making knock-in and knock-out alternations and thereby bring significant treatment outcomes in breast cancer have also been summarized.

摘要

乳腺癌是一种多因素的异质性疾病,是全球女性中第二常见的癌症。转移是这些患者最主要的死亡原因之一。早期或局部晚期乳腺癌局限于乳房或附近淋巴结。当乳腺癌从其原发部位扩散到更远的组织/器官时,就称为转移性或IV期乳腺癌。正常的乳腺发育受特定基因和控制细胞增殖、细胞死亡、细胞分化和细胞运动的信号通路调节。参与各种信号通路的基因失调不仅会导致原发性肿瘤的形成,还会导致转移。转移级联反应是一个多步骤过程,包括局部肿瘤细胞的侵袭,随后进入脉管系统,恶性细胞从循环中逸出并最终在远处部位定植。这些阶段分别称为原发性肿瘤形成、血管生成、侵袭、内渗和外渗。乳腺癌转移的主要部位是淋巴结、骨骼、大脑和肺部。据报道,IV期乳腺癌的五年生存率仅约为28%。转移是乳腺癌的一个严重问题,因此,已经开发了各种治疗策略,如酪氨酸激酶抑制剂,以靶向参与转移不同步骤的特定失调基因和各种信号通路。此外,高压氧疗法、RNA干扰和CRISPR/Cas9等其他疗法也正在作为治疗IV期/转移性乳腺癌的新策略进行探索。因此,本综述旨在评估IV期乳腺癌的遗传基础,重点关注分子机制。此外,还讨论了针对这些参与各种信号通路的失调基因的治疗策略。还总结了基因组编辑技术,这些技术可以通过进行敲入和敲除改变来靶向受影响区域的特定基因,从而在乳腺癌中带来显著的治疗效果。

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